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Anatomy Of A Riot – Outlook India

A blasphemous FB post, police inaction, a truculent SDPI and rumours of Congress infighting...all lead up to Bangalore's worst street rioting in yearsBy Ajay Sukumaran

August 31, 2020

Ground ZeroRiot police patrol a street in the violence-hit area of Bangalore. Photograph by PTI

No sooner had the August 11 mob violence in east Bangalores Kaval Byrasandra locality been containedafter police firing which claimed three livesthan the politics kicked in. The Congress hadnt reacted immediately and when it did, the response was guarded. So, leaders from the ruling BJP lost no time in prodding the party over appeasementthe violence-hit localities have a sizeable Muslim population and the Congress has a strong presence there. In fact, Congress MLA Akhanda Srinivasa Murthy, whose house was ransacked and burnt down, had won the 2018 polls with the highest vote share in Karnataka.

So what had gone wrong? A Facebook post on Prophet Muhammed shared by Murthys nephew P. Naveen touched off the riotous scenes in which a mob attacked his house, vandalised two police stations and torched vehicles on the street. But various undercurrents in these localitiesseemingly linked to the municipal polls that are due this yearalso appear to fill the frame of what has been Bangalores worst street riotings in several years. Karnatakas home minister Basavaraj Bommai hinted as...

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Anatomy Of A Riot - Outlook India

Irish Greys Anatomy star Richard Flood admits he was lucky to land role as hed been in LA five days when h – The Irish Sun

IRISH Grey's Anatomy star Richard Flood admitted that he was "lucky" to land the role in the hit series as he had only been in LA for five days when he got the good news.

Richard plays Dr. Cormac Hayes and he made his first appearance in the show last season.

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He got the good news recently that he would become a series regular and he revealed how he first landed the role.

The actor spoke on Ireland AM with hosts Simon Delaney and Glenda Gilson about the show.

Richard explained that he had been working on Shameless in LA for a couple of months before he decided to go visit his wife in Rome.

He spent seven months in Rome before he decided to go back to LA to see if he could get any gigs while he was there.

The actor explained: "So I finished Shameless and I'd been away from my family for five or six months when I was doing that.

"I went back to Rome, my wife was shooting a TV show she's an actress as well a very good actress.

"She was shooting that for seven months or something and by the end of that seven months I was like, 'Alright I need to go to LA and do something because I'm starting to go a little bit crazy even though I'm in Rome'."

Richard then went on to say that he decided to hop on a flight to LA and just a couple days later he landed the role on Grey's.

The actor explained: " I literally got on a plane to come out and see what was happening, see what was around and this time the timing was just right.

"I got off the plane on Friday I think and on Wednesday I was cast in Grey's so I just got lucky this time."

Richard also spoke about his day of filming admitting that he was "thrown" when he first got to the set but he "got stuck in".

The Dublin native said: "It all happened very quickly when I got out to LA. I was walking on not really knowing what I was walking into.

"It's kind of hard to take in especially a show like Grey's which is so famous it's been on for so long.

"You get a bit thrown at first but then you just get in and then you just have to start and you better get on with it that's it."

Richard went on to speak about his first meeting with Ellen Pompeo who stars in and directs the hugely popular series.

He said that she was great the first day they met and she spoke to him for an hour before he had even got the job.

Speaking on the Virgin Media show about Ellen, Richard said: "She's been great since the first day I met her.

"When I was just really meeting about the role, they were telling me about it, we had a really good chat for about an hour before I was even cast in the show.

"So I felt like we got to know each other and I knew what she was looking for and I knew where she was coming from.

"It's her show, she's been there for so long."

"I knew what they were looking for and I was just happy to get stuck in."

Simon and Glenda then asked Richard what the show will be like when it comes back and how they plan to adhere to the Covid restrictions.

He said: "I think we're lucky because Grey's has been around for so long that it's such a well-oiled machine now.

"Everyone really knows what they're doing and have done for years.

"So in a way, it's easier for us to get back up and running as fast as we have.

"So what it's looking like is the actors we're certainly going to be tested three times a week every week whether we're shooting or not.

"There's going to be a lot of scripts already ready so that if there is the unfortunate situation where there are some positive tests we'll be able to shift whatever we're shooting."

He explained that there will be different storylines in every episode in case something happens to one of the actors.

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Richard said: "There'll be lots of storylines running at the same time we'll be able to shoot whatever we can in case there are some positive tests.

"We're going to be kept in different pods, hair and makeup are going to be very different, camera crew are going to be kept at a distance and they're going to be wearing PPE the whole time.

"We're lucky as well that we're a medical show that it makes sense for us to have masks and PPE."

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Originally posted here:
Irish Greys Anatomy star Richard Flood admits he was lucky to land role as hed been in LA five days when h - The Irish Sun

Irish actor Richard Flood reveals he was cast in Grey’s Anatomy just days after he landed in LA – Goss.ie

Home Irish Showbiz Irish actor Richard Flood reveals he was cast in Greys Anatomy just...

The Dublin native has admitted he "got lucky"

Irish actor Richard Flood has revealed he was cast in Greys Anatomy just five days after he arrived in Los Angeles.

The 38-year-old landed the role ofDr. Cormac Hayes on the hit TV show last year, and hes since been made a series regular.

Speaking on Ireland AM, Richard said he had been living in Rome with his wife Gabriella for several months before he decided to return to LA.

Richard explained: My wife was shooting a TV show, shes an actress as well a very good actress. She was shooting that for seven months or something and by the end of that seven months I was like, Alright I need to go to LA and do something because Im starting to go a little bit crazy'

Richard said he hopped on a flight to LA, and just a couple days later he landed a role on Greys Anatomy.

I literally got on a plane to come out and see what was happening, see what was around and this time the timing was just right, he confessed.

I got off the plane on Friday I think and on Wednesday I was cast in Greys so I just got lucky this time.

Richard said he was immediately thrown into the deep end on his first day of shooting.

It all happened very quickly when I got out to LA. I was walking on not really knowing what I was walking into, he explained.

Its kind of hard to take in especially a show like Greys which is so famous its been on for so long. You get a bit thrown at first but then you just get in and then you just have to start and you better get on with it thats it.

Speaking about meeting the shows lead actress Ellen Pompeo, Richard said: Shes been great since the first day I met her.

When I was just really meeting about the role, they were telling me about it, we had a really good chat for about an hour before I was even cast in the show.

So I felt like we got to know each other and I knew what she was looking for and I knew where she was coming from. Its her show, shes been there for so long.

I knew what they were looking for and I was just happy to get stuck in, he added.

Originally posted here:
Irish actor Richard Flood reveals he was cast in Grey's Anatomy just days after he landed in LA - Goss.ie

Grey’s Anatomy star Jesse Williams’ new movie Random Acts of Violence is the goriest and most disgusting of 2020 – digitalspy.com

With a title like Random Acts of Violence, you're not exactly expecting a family-friendly affair, but you might not be expecting just how violent these random acts get.

Directed by Jay Baruchel (the voice of Hiccup from How to Train Your Dragon, lest we forget) and on Shudder now, the movie based on the comic book of the same name sees Grey's Anatomy star Jesse Williams play Todd Walkley, who is struggling to find a way to end his comic book SLASHERMAN.

Todd sets off on a road trip with his wife Kathy (Fast & Furious star Jordana Brewster), assistant Aurora (Niamh Wilson) and best friend/publisher Ezra (Baruchel) to New York Comic-Con, hoping that he'll solve his creative dilemma along the way.

What he doesn't expect is to be trailed by a series of grotesque murders, seemingly inspired by the deaths in his own comic book and things soon get really bloody, really fast.

Shudder/Elevation Pictures

Watch Random Acts of Violence on Shudder

For a movie with a runtime of around 80 minutes, Random Acts of Violence sure packs a lot into its brief stay. It's smarter and sharper than you'd expect from its bloody concept, so you could almost say it has a brain to go with its literal brains on display.

One of the reasons Todd wants to end his successful comic book is that he's dismayed with the continued violence in it, especially since SLASHERMAN was inspired by real-life murders with genuine victims whose families were forever affected by their loss.

When the real-life murders start up again, Todd is forced to assess his responsibility for the killing spree. Would they have happened even if he didn't publish his comic book? How much of an effect does art have on real life?

It's a meaty subject and while Random Acts of Violence addresses it, it certainly offers no easy answers. There's also a fine balancing act on display too, as in telling its story, the movie offers some extremely graphic violence of its own.

We're not being dramatic when we say the movie is set to be the goriest and most disgusting of 2020, one that even the most hardened gore hounds might not want to watch while eating.

Not only are the killings graphic, but the killer's signature touch is to leave their victims in gruesome displays that they believe is their art. Think Hannibal, just with more blood.

The effects on display are truly impressive and gut-churning, whether it's an unforgettable 'threesome' or the most messed-up family Christmas dinner ever. You'll both want to look away and applaud the work.

With most of the crimes committed against women though, it feels at times though that Random Acts of Violence wants to have its cake and eat it too. There's a hypothetical version of this movie that could have been made without the need for the bloody violence and macabre displays. It could be argued that the movie is doing the exact thing that it seems to be criticising.

Equally, by making it hard to watch and so extreme, does that make its point more effective? By confronting us with it in its rawest form, it forces you to think about your reaction to the violence.

"I've wondered a lot how much this idea of 'the woman as victim' had been sort of drilled into my subconscious, from music videos to victims in horror movies," Baruchel told The Independent in a recent interview.

"I could name the Zodiac Killer and John Wayne Gacy, but almost none of the people they killed. I could name Freddy and Jason and Michael Myers, but none of their victims on screen. What the f**k is that?"

Baruchel recalled the debate around the Columbine shootings when Marilyn Manson's music was being blamed, while artists were defending their right to make art about anything without social consequence.

"But once you put that out there, once you engage in a debate with a stranger, or on Twitter, or you put up a poster, I believe you are somewhat connected to that, and you are somewhat responsible. There are consequences to putting shit out," he added.

Shudder/Elevation Pictures

To that extent, he likely will relish the debate that Random Acts of Violence is sure to provoke in terms of whether it goes too far in displaying the very thing it aims to criticise.

You can say what you want about it, but the movie certainly isn't easy to forget.

Random Acts of Violence is available to watch now on Shudder.

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Grey's Anatomy star Jesse Williams' new movie Random Acts of Violence is the goriest and most disgusting of 2020 - digitalspy.com

‘Grey’s Anatomy’ Will Have the Most Mask Compliance of Any Film Set This Fall – Showbiz Cheat Sheet

Like so many projects on television,Greys Anatomy was cut short by four episodes due to the coronavirus pandemic and the dangers of everyone being on set together.

The decision was made to simply end Season 16 and move on to Season 17 this fall, just to be safe. Several storylines were never wrapped up, including romantic entanglements, whether or not some characters would return to the show, and if the show will tackle the pandemic at all in the next episodes.

Showrunner Krista Vernoff address this and more as actors tease the continuance of production happening in the next few weeks.

The writers room atGreys Anatomy includes a group they refer to as Team Medical, according to Vernoff. Theyre medical professionals that consult on the show to try to keep the medicine as true to real life as possible. They convinced Vernoff and the other writers that it would be irresponsible to leave out the story of the pandemic.

Theres a lot to address, though, and Vernoff says of the challenge via Deadline: How do we do that and provide some escapism? How do we do that and create romance, and comedy, and joy, and fun?

Vernoff implied that the stories that were cut short at the end of Season 16 would still be picked back up, but without the physical contact weve seen in the past.

Instead of fevered make-out sessions and heavy breathing, itll be more subtle but still sexy. Theyll have to play around with the camera angles and placement of actors in order to show what they want to but the implication was that fans should be excited.

In the past, Ellen Pompeo teased that her character, the iconic Meredith Grey would be leaving the show but now she teases Merediths return.

During all the controversy over masks, fans wondered if the show would address the issue of anti-maskers. The teasers and rumors for the show say that they have no intention of getting political.

Being a medical show that has people wearing medical-grade masks regularly, it will be easy for the show to start back up with everyone wearing masks all the time on set. But thats as far as the writers are willing to go when it comes to addressing masks in the shows plot.

Meredith faced jail time for her activism in season 16. It appears that Kevin McKidds character Dr. Owen Hunt will have a bigger role to play in the pandemic storyline of season 17. His character went through a war and lives with PTSD. Vernoff talked about how those skills will come into play with this new story.

RELATED: Greys Anatomy: Some Fans are Ready For the Series to End

What became the season 16 finale was the episode where Teddy and Owen were supposed to get married. Owen heard the accidental voicemail where Teddy and Dr. Tom Koracick were supposedly ending their affair. Theres a lot of heavy breathing and obvious noises with an ending of Tom asking Teddy to run away with him.

Vernoff revealed that those last four episodes that didnt get filmed were supposed to revolve heavily around the Teddy Owen Tom triangle. With mask compliance being a big deal when the show continues production, those stories may have to change.

It was confirmed that Carina DeLucas character would leave the show after her and Station 19s Maya Bishop solidified their relationship.

Series regular Amelia Shepherd had her baby with Dr. Atticus Link Lincoln and the birth process didnt go as planned at all. Even Merediths half-sister and head of the cardio thoracic surgery department Dr. Margaret Pierce (a.k.a Maggie) has a love interest.

All of these romances are set to return but with mask compliance in place on set. Fans will have to wait a few weeks more to find out what that will look like.

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'Grey's Anatomy' Will Have the Most Mask Compliance of Any Film Set This Fall - Showbiz Cheat Sheet

New tools catch and release cellular targets at the flip of a light switch – Princeton University

A Princeton team has developed a class of light-switchable, highly adaptable molecular tools with new capabilities to control cellular activities. The antibody-like proteins, called OptoBinders, allow researchers to rapidly control processes inside and outside of cells by directing their localization, with potential applications including protein purification, the improved production of biofuels, and new types of targeted cancer therapies.

This time-lapse movie shows a new tool called an OptoBinder that can latch onto and release molecules in response to light. In this case, a fluorescent OptoBinder is attaching to actin, a component of cells key to their structure and shape. The OptoBinder strongly binds to actin in the dark, but releases its hold in the presence of blue light (indicated by blue box at top right).

Video courtesy of the researchers; GIF by Bumper DeJesus

In a pair of papers published Aug. 13 in Nature Communications, the researchers describe the creation of OptoBinders that can specifically latch onto a variety of proteins both inside and outside of cells. OptoBinders can bind or release their targets in response to blue light. The team reported thatone type of OptoBinderchanged its affinity for its target molecules up to 330-fold when shifted from dark to blue light conditions, whileothersshowed a five-fold difference in binding affinity all of which could be useful to researchers seeking to understand and engineer the behaviors of cells.

Crucially, OptoBinders can target proteins that are naturally present in cells, and their binding is easily reversible by changing light conditions a new capability that is not available to normal antibodies, said co-authorJos Avalos, an assistant professor ofchemical and biological engineeringand theAndlinger Center for Energy and the Environment. The ability to let go [of a target protein] is actually very valuable for many applications, said Avalos, including engineering cells metabolisms, purifying proteins or potentially making biotherapeutics.

The new technique is the latest in a collaboration between Avalos andJared Toettcher, an assistant professor ofmolecular biology. Both joined the Princeton faculty in 2015, and soon began working together on new ways to applyoptogenetics a set of techniques that introduce genes encoding light-responsive proteins to control cells behaviors.

We hope that this is going to be the beginning of the next era of optogenetics, opening the door to light-sensitive proteins that can interface with virtually any protein in biology, either inside or outside of cells, said Toettcher, the James A. Elkins, Jr. 41 Preceptor in Molecular Biology.

The research team included (from left) Jos Avalos, an assistant professor of chemical and biological engineering and the Andlinger Center for Energy and the Environment; associate research scholar Csar Carrasco-Lpez; assistant professor of molecular biology Jared Toettcher; and postdoctoral research fellow Agnieszka Gil.

Avalos and his team hope to use OptoBinders to control the metabolisms of yeast and bacteria to improve the production of biofuels and other renewable chemicals, while Toettchers lab is interested in the molecules potential to control signaling pathways involved in cancer.

The two papers describe different types of light-switchable binders: opto-nanobodies and opto-monobodies. Nanobodies are derived from the antibodies of camelids, the family of animals that includes camels, llamas and alpacas, which produce some antibodies that are smaller (hence the name nanobody) and simpler in structure than those of humans or other animals.

Nanobodies small size makes them more adaptable and easier to work with than traditional antibodies; they recently received attention for their potential as a COVID-19 therapy. Monobodies, on the other hand, are engineered pieces of human fibronectin, a large protein that forms part of the matrix between cells.

These papers go hand in hand, said Avalos. The opto-nanobodies take advantage of the immune systems of these animals, and the monobodies have the advantage of being synthetic, which gives us opportunities to further engineer them in different ways.

The two types of OptoBinders both incorporate a light-sensitive domain from a protein found in oat plants.

When you turn the light on and off, these tools bind and release their target almost immediately, so that brings another level of control that was not previously possible, said co-author Csar Carrasco-Lpez, an associate research scholar in Avalos lab. Whenever you are analyzing things as complex as metabolism, you need tools that allow you to control these processes in a complex way in order to understand what is happening.

When you turn the light on and off, these tools bind and release their target almost immediately, so that brings another level of control that was not previously possible, said co-author Csar Carrasco-Lpez, an associate research scholar in Avalos lab.

In principle, OptoBinders could be engineered to target any protein found in a cell. With most existing optogenetic systems, you always had to genetically manipulate your target protein in a cell for each particular application, said co-author Agnieszka Gil, a postdoctoral research fellow in Toettchers lab. We wanted to develop an optogenetic binder that did not depend on additional genetic manipulation of the target protein.

In a proof of principle, the researchers created an opto-nanobody that binds to actin, a major component of the cytoskeleton that allows cells to move, divide and respond to their environment. The opto-nanobody strongly bound to actin in the dark, but released its hold within two minutes in the presence of blue light. Actin proteins normally join together to form filaments just inside the cell membrane and networks of stress fibers that traverse the cell. In the dark, the opto-nanobody against actin binds to these fibers; in the light, these binding interactions are disrupted, causing the opto-nanobody to scatter throughout the cell. The researchers could even manipulate binding interactions on just one side of a cell a level of localized control that opens new possibilities for cell biology research.

OptoBinders stand to unlock scores of innovative, previously inaccessible uses in cell biology and biotechnology, said Andreas Mglich, a professor of biochemistry at the University of Bayreuth in Germany who was not involved in the studies. But, Mglich said, there is much more to the research because the design strategy can be readily translated to other molecules, paving the way to an even wider repertoire of customized, light-sensitive binders.

The impressive results mark a significant advance, he said.

Future applications will depend on being able to generate more OptoBinders against a variety of target proteins, said Carrasco-Lpez. We are going to try to generate a platform so we can select OptoBinders against different targets using a standardized, high-throughput protocol, he said, adding that this is among the first priorities for the team as they resume their experiments after lab research was halted this spring due to COVID-19.

Beyond applications that involve manipulating cell metabolism for microbial chemical production, Avalos said, OptoBinders could someday be used to design biomaterials whose properties can be changed by light.

The types of OptoBinders developed by postdoctoral research fellow Agnieszka Gil and colleagues could in principle be engineered to target any protein in a cell, opening new possibilities for fundamental research, biofuel production and therapeutics.

The technology also holds promise as way to reduce side effects of drugs by focusing their action to a specific site in the body or adjusting dosages in real time, said Toettcher, who noted that applying light inside the body would require a device such as an implant. There arent many ways to do spatial targeting with normal pharmacology or other techniques, so having that kind of capability for antibodies and therapeutic binders would be a really cool thing, he said. We think of this as a sea change in what sorts of processes can be placed under optogenetic control.

Other authors on the opto-monobody paper were Evan Zhao, who earned a Ph.D. in chemical and biological engineering from Princeton in 2019; and Nathan Alam, an undergraduate from the Class of 2021. Zhao was also a co-author on the opto-nanobody paper, along with Liyuan Zhu, a graduate student in the Department of Chemistry; Pavithran Ravindran, a research specialist in molecular biology; Maxwell Wilson, a former associate research scholar in molecular biology who is now an assistant professor at the University of California-Santa Barbara; and Alexander Goglia, a medical student in the Robert Wood Johnson Medical School and Princeton University M.D./Ph.D. program.

The work was supported in part by the U.S. National Institutes of Health, National Science Foundation and Department of Energy; the Pew Charitable Trusts; and the Eric and Wendy Schmidt Transformative Technology Fund.

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New tools catch and release cellular targets at the flip of a light switch - Princeton University

Covid-19 Impact on Global Cell Biology Cloud Computing Market 2020 by Company, Type and Application, Forecast to 2025 – The Daily Chronicle

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Covid-19 Impact on Global Cell Biology Cloud Computing Market 2020 by Company, Type and Application, Forecast to 2025 - The Daily Chronicle

Better Tool Created to Aid COVID-19 Diagnosis – SciTechDaily

An LSU Health New Orleans radiologist and evolutionary anatomist have teamed up to show the same techniques used for research on reptile and bird lungs can be used to help confirm the diagnosis of COVID-19 in patients. Their paper published in BMJ Case Reports demonstrates that 3D models are a strikingly clearer method for visually evaluating the distribution of COVID-19-related infection in the respiratory system. Credit: LSU Health New Orleans

A Louisiana State University Health New Orleans radiologist and evolutionary anatomist have teamed up to show the same techniques used for research on reptile and bird lungs can be used to help confirm the diagnosis of COVID-19 in patients. Their paper published in BMJ Case Reports demonstrates that 3D models are a strikingly clearer method for visually evaluating the distribution of COVID-19-related infection in the respiratory system.

Emma R. Schachner, PhD, Associate Professor of Cell Biology & Anatomy, and Bradley Spieler, MD, Vice Chairman of Radiology Research and Associate Professor of Radiology, Internal Medicine, Urology, & Cell Biology and Anatomy at LSU Health New Orleans School of Medicine, created 3D digital models from CT scans of patients hospitalized with symptoms associated with severe acute respiratory syndrome coronavirus (SARS-CoV-2).

Three patients who were suspected of having COVID-19 underwent contrast enhanced thoracic CT when their symptoms worsened. Two had tested positive for SARS-CoV-2, but one was reverse transcription chain reaction (RT-PCR) negative. But because this patient had compelling clinical and imaging, the result was presumed to be a false negative.

An array of RT-PCR sensitivities has been reported, ranging from 30-91%, notes Dr. Spieler. This may be the result of relatively lower viral loads in individuals who are asymptomatic or experience only mild symptoms when tested. Tests performed when symptoms were resolving have also resulted in false negatives, which seemed to be the result in this case.Given diagnostic challenges with respect to false negative results by RT-PCR, the gold standard for COVID-19 diagnostic screening, CT can be helpful in establishing this diagnosis. Importantly, these CT features can range in form and structure and appear to correlate with disease progression. This allows for 3D segmentation of the data in which lung tissue can be volumetrically quantified or airflow patterns could be modeled.

The CT scans were all segmented into 3D digital surface models using the scientific visualization program Avizo (Thermofisher Scientific) and techniques that the Schachner Lab uses for evolutionary anatomy research.The full effect of COVID-19 on the respiratory system remains unknown, but the 3D digital segmented models provide clinicians a new tool to evaluate the extent and distribution of the disease in one encapsulated view, adds Spieler. This is especially useful in the case where RT-PCR for SARS-CoV-2 is negative but there is strong clinical suspicion for COVID-19.

To date, there havent been good models of what COVID is doing to the lungs. So, this project focused on the visualization of the lung damage in the 3D models as compared to previous methods that have been published volume-rendered models and straight 2D screen shots of CT scans and radiographs.Previously published 3D models of lungs with COVID-19 have been created using automated volume rendering techniques, says Dr. Schachner. Our method is more challenging and time-consuming, but results in a highly accurate and detailed anatomical model where the layers can be pulled apart, volumes quantified, and it can be 3D printed.

The three models all show varying degrees of COVID-19 related infection in the respiratory tissues particularly along the back of the lungs, and bottom sections. They more clearly show COVID-19-related infection in the respiratory system compared to radiographs (x-rays), CT scans, or RT-PCR testing alone. Schachner and Spieler are now segmenting more models for a larger follow-up project.

Reference: Three-dimensional (3D) lung segmentation for diagnosis of COVID-19 and the communication of disease impact to the public by Emma R Schachner and Bradley Spieler, 18 August 2020, BMJ Case Reports.DOI: 10.1136/bcr-2020-236943

Link:
Better Tool Created to Aid COVID-19 Diagnosis - SciTechDaily

Researchers Identify Enzyme Linked to Colitis – Rutgers Today

Rutgers-Newark study may help develop future treatments for inflammatory bowel disease Nan Gao, associate professor of cell biology in the Department of Biological Sciences, School of Arts and Sciences-Newark, discovered that an enzyme, which should stop bacterial growth in the digestive tract, instead stimulates inflammation in people with colitis.

Devyn Nunez, Shine Portrait Studio

An enzyme that usually stops bacterial growth in the large intestine stimulates inflammation in some people, resulting in ulcerative colitis a chronic digestive disease that affects more than 750,000 Americans, according to scientists at Rutgers University-Newark.

In a new study published inImmunity, lead author Nan Gao, associate professor of cell biology in the Department of Biological Sciences, School of Arts and Sciences-Newark, reports that in people with ulcerative colitis, the gut enzyme lysozyme, which normally functions to restrain bacterial growth, instead stimulates inflammation.

This results in the formation of ulcers and sores in the large intestine and rectum, hallmarks of the inflammatory bowel disease. Detecting these cells in the inner lining of the colon and rectum is a standard diagnostic feature of chronic intestinal inflammation.

This study demonstrated the existence of a delicate balance between inflammatory and anti-inflammatory factors in our intestines, said Gao, who conducted it with postdoctoral researcher Richard Yu and doctoral student Iyshwarya Balasubramanian. Insights about how to gain such beneficial immune balance may be useful for future intervention of inflammatory bowel disease.

In biochemical and genetic mouse laboratory studies, Gao and his team focused on Paneth cells, the main producers of lysozyme, which are typically found in the small intestine and rarely observed in the large intestine or healthy colon. In cases of patients with inflammatory bowel disease, which affects 1.6 million people in the United States, Paneth cells are often seen in the colon and rectum.

The frequent appearance of Paneth cells in the inflamed tissues of patients' colons is highly unusual and poorly understood, Gao said.

In the Rutgers-Newark study, scientists discovered that lysozyme secreted by Paneth cells located in colon results in suppressing the growth of certain bacterial species and results in an imbalance in the gut microbiome, which leads to intestinal inflammation.

In healthy individuals that have normal production of gut lysozyme, these bacteria flourish enabling an individual immune response that prevents colitis.

This delicate balance is achieved and maintained by a constant interaction between our body and the commensal microorganisms that play a significant role in digestion, metabolism, and the immune system, Gao said.

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Researchers Identify Enzyme Linked to Colitis - Rutgers Today

3D Cell Cultures Industry Report 2020-2025: Impact of COVID-19 on the World of Cell Culture – PRNewswire

DUBLIN, Aug. 19, 2020 /PRNewswire/ -- The "3D Cell Cultures: Technologies and Global Markets" report has been added to ResearchAndMarkets.com's offering.

The report includes:

Whether the discussion is about stem cells, tissue engineering, or microphysiological systems, their vital role in drug discovery, toxicology, and other areas leading to new product development, 3D cell culture is becoming the environment that will increasingly define the basis for future advances.

To mix metaphors, 3D cell culture is also cross-roads through which just about everything else passes on its way to building knowledgebases or introducing new products. This study is needed to bring together and make sense out of the broad body of information encompassed by 3D cell culture.

Three-dimensional cell culture has been used by researchers for many years now, with early adoption and now key roles in cancer and stem cells. Organ-on-a-chip technology, also known as microphysiological systems, is leading to dramatic breakthroughs. Also, stem cell research coupled with synthetic biology is opening new areas. This study is needed to provide a perspective on these advances.

Furthermore, classical toxicology testing programs have been in place for many decades, and over the past 20 years, animal welfare and scientific activities have spurred the development of in vitro testing methods. In silico methods are advancing in novel ways that need to be analyzed and considered in terms of their impacts on cell culture.

This report investigates the recent key technical advances in 3D cell culture equipment, raw materials, assay kits, analytical methods, and clinical research organization (CRO) services. It should also be pointed out that this report takes a somewhat different position on 2D cell culture. It has been criticized for its inadequacies and the misleading information it can produce. However, a review of industry practices makes it clear that it still has its place and will contribute to future advances in unexpected ways.

The company section looks at many of the suppliers who provide equipment, assays, cells, reagents, and services used in 3D cell culture. This study sought to understand business models and market maturity dynamics in greater depth as well as providing more quantitative analysis of their operations.

Key Topics Covered

Chapter 1 Introduction

Chapter 2 Summary

Chapter 3 Highlights and Issues

Chapter 4 Tissue and Cell Culture: Technology and Product Background

Chapter 5 Assays, Imaging and Analysis

Chapter 6 Regulation and Standardization

Chapter 7 3D Models for Cancer

Chapter 8 Landscape for Toxicology and Drug Safety Testing

Chapter 9 Stem Cell Landscape

Chapter 10 Regenerative Medicine: Organ Transplants and Skin Substitutes

Chapter 11 Company Profiles

For more information about this report visit https://www.researchandmarkets.com/r/jesu26

Research and Markets also offers Custom Research services providing focused, comprehensive and tailored research.

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3D Cell Cultures Industry Report 2020-2025: Impact of COVID-19 on the World of Cell Culture - PRNewswire